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Dive into the research topics where Kumie Nojima is active.

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Featured researches published by Kumie Nojima.


International Journal of Radiation Oncology Biology Physics | 2001

Preclinical biological assessment of proton and carbon ion beams at Hyogo Ion Beam Medical Center

Kazufumi Kagawa; Masao Murakami; Yoshio Hishikawa; Mitsuyuki Abe; Takashi Akagi; Toshihiro Yanou; Gou Kagiya; Yoshiya Furusawa; Koichi Ando; Kumie Nojima; Mizuho Aoki; Tatsuaki Kanai

PURPOSE To assess the biologic effects of proton and carbon ion beams before clinical use. METHODS AND MATERIALS Cultured cells from human salivary gland cancer (HSG cells) were irradiated at 5 points along a 190 MeV per nucleon proton and a 320 MeV per nucleon carbon ion beam, with Bragg peaks modulated to 6 cm widths. A linac 4 MV X-ray was used as a reference. Relative biologic effectiveness (RBE) values at each point were calculated from survival curves. Cells were also irradiated in a cell-stack phantom to identify that localized cell deaths were observed at predefined depth. Total body irradiation of C3H/He mice was performed, and the number of regenerating crypts per jejunal section was compared to calculate intestinal RBE values. For carbon ion and referential 4 MV X-ray beams, mouse right legs were irradiated by four-fractional treatment and followed up for skin reaction scoring. RESULTS RBE values calculated from cell survival curves at the dose that would reduce cell survival to 10% (D10) ranged from 1.01 to 1.05 for protons and from 1.23 to 2.56 for carbon ions. The cell-stack phantom irradiation revealed localized cell deaths at predefined depth. The intestinal RBE values ranged from 1.01 to 1.08 for protons and from 1.15 to 1.88 for carbon ions. The skin RBE value was 2.16 at C320/6 cm spread-out Bragg peak (SOBP) center. CONCLUSION The radiobiologic measurements of proton and carbon ion beams at Hyogo Ion Beam Medical Center are consistent with previous reports using proton beams in clinical settings and carbon ion beams with similar linear energy transfer (LET) values.


Cancer Research | 2005

Extremely Low Dose Ionizing Radiation Up-regulates CXC Chemokines in Normal Human Fibroblasts

Akira Fujimori; Ryuichi Okayasu; Hiroshi Ishihara; Satoshi Yoshida; Kiyomi Eguchi-Kasai; Kumie Nojima; Satoru Ebisawa; Sentaro Takahashi

Although the public today could be exposed to X-rays as high as 1 cGy due to diagnostic procedures, the biological effects of this low-dose range have not been well established. We searched through >23,000 transcripts in normal human fibroblasts, HFLIII, using a novel comprehensive expression analysis method. More than 200 genes were up-regulated transiently by 1 cGy of X-rays during the 1-hour period after irradiation. We determined the nucleotide sequence of 10 up-regulated transcripts with the greatest rate of increase in the irradiated HFLIII cells. Three of the 10 transcripts encoded CXC chemokines (CXCL1, CXCL2, and CXCL6). The rest included the transcripts of other secretory products (secretogranin II, thrombospondin type I domain containing 2, amphiregulin, and interleukin-6) and unknown genes. To test the involvement of CXC chemokines in cells irradiated with low doses, we irradiated HFLIII cells with 1 to 20 cGy X-rays and transferred the media from HFLIII culture to two melanoma cell lines characteristic of excessive numbers of the CXC chemokine-specific receptors. The growth of these melanoma lines were significantly stimulated by the medium from HFLIII irradiated at 1 to 5 cGy. Our results indicate that human cells respond to doses of radiation as low as 1 cGy, and mechanisms alternative to those involved in moderate/high-dose studies have to be considered in understanding the biological effects of diagnostic level radiation. In addition, our comprehensive approach using a novel expression profiling method is a powerful strategy to explore biological functions associated with very low levels of toxic agents.


Cancer Letters | 1998

Evidence for mRNA expression of vascular endothelial growth factor by X-ray irradiation in a lung squamous carcinoma cell line

Soichiro Ando; Kumie Nojima; Hideyuki J. Majima; Hiroshi Ishihara; Masao Suzuki; Yoshiya Furusawa; Hiroshi Yamaguchi; Sachiko Koike; Koichi Ando; Masatake Yamauchi; Takayuki Kuriyama

Vascular endothelial growth factor (VEGF) is a multipotent cytokine which plays an important role in various angiogenic conditions as well as in some tumor behaviors. Here we examined the induction of VEGF mRNA by X-ray irradiation in a lung squamous cell carcinoma cell line (RERF-LC-AI). Irradiating the cells with 15 Gy X-rays significantly increased the mRNA expression up to 2.5-fold of control at a post-irradiation time of 16-24 h. The induction of VEGF mRNA by X-ray irradiation was completely blocked by treating cells with either genistein (Src tyrosine kinase inhibitor) or H7 (protein kinase C inhibitor). This suggests that the mechanism of induction might be concerned with the pathway which triggers Src tyrosine kinase of the cell surface and the protein kinase C pathway.


Trends in Biotechnology | 2014

Caution required for handling genome editing technology

Motoko Araki; Kumie Nojima; Tetsuya Ishii

Genome-editing technology, although a robust tool for genetic engineering, is creating indistinct regulatory boundaries between naturally occurring and modified organisms. However, researchers must act with caution in research and development to avoid misleading society. Furthermore, appropriate regulations should be proactively discussed and established for handling genome-editing technology.


Proceedings of the National Academy of Sciences of the United States of America | 2005

Germ cell mutagenesis in medaka fish after exposures to high-energy cosmic ray nuclei: A human model

Atsuko Shimada; Akihiro Shima; Kumie Nojima; Yo Seino; Richard B. Setlow

Astronauts beyond the Earths orbit are exposed to high-energy cosmic-ray nuclei with high values of linear energy transfer (LET), resulting in much more biological damage than from x-rays or γ-rays and may result in mutations and cancer induction. The relative biological effectiveness of these nuclei depends on the LET, rising to as high as ≈50 at LET values of ≈100-200 keV/μm. An endpoint of concern is germ cell mutations passed on to offspring, arising from exposure to these nuclei. A vertebrate model for germ cell mutation is Medaka fish (Oryzias latipes). We exposed wild type males to doses of 1 GeV per nucleon Fe nuclei or to 290 MeV per nucleon C nuclei. They were mated to females with recessive mutations at five-color loci. The transparent embryos from >100 days of mating (representing exposed sperm, spermatids, or spermatogonia) were observed so as to detect dominant lethal mutations and total color mutations, even though the embryos might not hatch. The relative number of mutant embryos as a function of dose were compared with those induced by γ-rays. The relative biological effectiveness values for dominant lethal mutations and total color mutations for exposed sperm and spermatids were 1.3-2.1 for exposure to C nuclei and 1.5-3.0 for exposure to Fe nuclei. (The spermatogonial data were uncertain.) These low values, and the negligible number of viable mutations, compared with those for mutations in somatic cells and for neoplastic transformation, indicate that germ cell mutations arising from exposures to cosmic ray nuclei are not a significant hazard to astronauts.


Radiation Research | 2005

Effects of Prenatal Irradiation with an Accelerated Heavy-Ion Beam on Postnatal Development in Rats: I. Neurophysiological Alterations

Bing Wang; Masahiro Murakami; Kiyomi Eguchi-Kasai; Kumie Nojima; Yi Shang; Kaoru Tanaka; Kazuko Fujita; Hervé Coffigny

Abstract Wang, B., Murakami, M., Eguchi-Kasai, K., Nojima, K., Shang, Y., Tanaka K., Fujita, K., Coffigny, H. and Hayata, I. Effects of Prenatal Irradiation with an Accelerated Heavy-Ion Beam on Postnatal Development in Rats: I. Neurophysiological Alterations. Radiat. Res. 164, 561–566 (2005). Effects on postnatal neurophysiological development in offspring were studied after exposure of pregnant Wistar rats to accelerated carbon-ion beams with an LET of about 13 keV/ μm at doses ranging from 0.1 Gy to 2.5 Gy on the 15th day of gestation. The age at which four physiological markers appeared and five reflexes were acquired was examined prior to weaning. Gain in body weight was monitored until the offspring were 3 months old. Male offspring were evaluated as young adults using two behavioral tests. The effects of X rays estimated for the same biological end points were studied for comparison. For most of the end points at early age, no significant alterations were observed in offspring that received prenatal irradiation with 0.1 Gy of either accelerated carbon ions or X rays compared to the offspring of sham-irradiated dams. However, all offspring whose dams received 2.5 Gy died prior to weaning. Offspring from dams irradiated with accelerated carbon ions generally showed higher incidences of prenatal death and preweaning mortality, markedly delayed accomplishment in their physiological markers and reflexes, and gain in body weight compared to those exposed to X rays at doses of 0.5 to 2 Gy. Significantly reduced ratios of main organ weight to body weight at the postnatal ages of 30, 60 and 90 days were also observed within this dose range. The results indicate that irradiation with 0.5 to 2 Gy on day 15 of gestation caused permanent alterations in offspring that were dependent on dose. The alterations include permanent growth retardation, morphological malformations in main organs, including microcephaly, diminished reflex attainment, delayed appearance of physiological markers, and changes in adult behavior. Exposure to 1 to 2 Gy of radiation resulted in growth retardation and behavioral alterations that persisted throughout life. Accelerated carbon ions generally induced more detrimental effects than X rays.


Advances in Space Research | 2000

Effects of carbon ions on primary cultures of mouse brain cells

Kumie Nojima; Koichi Ando; H. Fujiwara; S. Ando

Primary mixed cultures of astrocytes and microglia were obtained from neonatal mice, and were irradiated with high-LET carbon ions. Immunohistochemical staining showed astrocytes survived more prominently than microglia. Tagged with specific antibodies, astrocytes and microglia surviving after irradiation were counted by flow cytometry. Decreases in the number of microglia and astrocytes were detected at a dose as small as 2 Gy when Day 5 cultures were irradiated with 13 keV/micrometer carbon ions. When the cultures were irradiated on Day 10, the dose-dependent decrease of microglia was more prominent for 13 keV/micrometer carbon ions than 70 keV/micrometer carbon ions. Astrocytes showed a marginal decrease at Day 10 and Day 14. We concluded that microglia are more sensitive than astrocytes to carbon ions and X-rays, and that the radiosensitivity of microglia depends on both differentiation/proliferation status and radiation quality.


Cancer Research | 2005

Particle Irradiation Suppresses Metastatic Potential of Cancer Cells

Toshiyuki Ogata; Teruki Teshima; Kazufumi Kagawa; Yoshio Hishikawa; Yutaka Takahashi; Atsuko Kawaguchi; Yuko Suzumoto; Kumie Nojima; Yoshiya Furusawa; Nariaki Matsuura


Proceedings of the National Academy of Sciences of the United States of America | 1997

Calorie restriction reduces the incidence of myeloid leukemia induced by a single whole-body radiation in C3H/He mice

Kazuko Yoshida; Tohru Inoue; Kumie Nojima; Yoko Hirabayashi; Toshihiko Sado


Journal of Radiation Research | 2001

Relative Biological Effectiveness of the 235 MeV Proton Beams at the National Cancer Center Hospital East

Koichi Ando; Yoshiya Furusawa; Masao Suzuki; Kumie Nojima; Hideyuki J. Majima; Sachiko Koike; Mizuho Aoki; Wakako Shimizu; Yasuyuki Futami; Takashi Ogino; Shigeyuki Murayama; Hiroshi Ikeda

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Koichi Ando

National Institute of Radiological Sciences

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Sachiko Koike

National Institute of Radiological Sciences

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Yoshiya Furusawa

National Institute of Radiological Sciences

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Nobuhiko Takai

National Institute of Radiological Sciences

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Shunji Nagaoka

Fujita Health University

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Chisa Oohira

National Institute of Radiological Sciences

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Manami Monobe

Tokyo University of Science

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Masao Suzuki

National Institute of Radiological Sciences

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Mizuho Aoki

National Institute of Radiological Sciences

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